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. 2017 Jan 25;37(4):1039–1054. doi: 10.1523/JNEUROSCI.1647-16.2016

Table 1.

Additional compounds tested on P23H rhodopsin-transgenic X. laevis and results obtained

Compound Category Concentrations tested n p-valuea Most effective concentration
VPA MS, GSK3I, CC, HDACi 1, 3, 10 μmb 13–15 1.5 × 10−12 10 μm
Valpromide MS, SA 0.1, 0.3, 0.5, 1 mm 6–11 NS
Valnoctamide MS, SA 0.5 mm 10–15 NS
Lithium chloride MS, GSK3I 0.3, 1 mmb 13–15 NS
Carbamazepine MS 100 μmb 7–12 NS
4-PBA CC 3, 10, 30 μmb 11–16 NS
Curcumin CC 333 μmb 7–9 NS
Sodium butyrate HDACi 10, 30, 100, 300 μmb 8–9 0.0022 300 μm
Vorinostat HDACi 3, 10, 30, 100 μmb 6–7 0.007 30 μm
CI-994 HDACi 0.2, 0.6, 2, 6, 19, 37, 56 μmc 7–10 4.5 × 10−13 56 μmd

ap-value associated with one-way ANOVA in an experiment comparable to that shown in Figure 1. For compounds tested at a single concentration, a t test (treated vs untreated) was used. p > 0.05, NS.

bHigher concentrations were toxic.

cHighest readily achievable concentration.

dAlthough 56 μm resulted in the highest total rod opsin levels, it did show some toxicity, so 37 μm was used in Figure 5IK.

SA, Structural analog of VPA; MS, mood stabilizer; CC, chemical chaperone; GSK3I, glycogen synthase kinase 3 inhibitor.